Molecular Characterization of Human Papillomavirus Type 159 (HPV159)

• Main Authors: Iva Marković, Lea Hošnjak, Katja Seme, Mario Poljak
• Format: Article
• Language: English
• Published: MDPI AG 2021-08-01
• Series: Viruses
• Subjects: human papillomavirus; <i>Betapapillomavirus</i>; phylogenetic characterization; viral load; prevalence; tissue tropism
• Online Access: https://www.mdpi.com/1999-4915/13/8/1668

Human papillomavirus type 159 (HPV159) was identified in an anal swab sample and preliminarily genetically characterized by our group in 2012. Here we present a detailed molecular in silico analysis that showed that the HPV159 viral genome is 7443 bp in length and divided into five early and two late genes, with conserved functional domains and motifs, and a non-coding long control region (LCR) with significant regulatory sequences that allow the virus to complete its life cycle and infect novel host cells. HPV159, clustering into the cutaneotropic <i>Betapapillomavirus</i> (<i>Beta</i>-PV) genus, is phylogenetically most similar to HPV9, forming an individual phylogenetic group in the viral species <i>Beta</i>-2. After testing a large representative collection of clinical samples with HPV159 type-specific RT-PCR, in addition to the anal canal from which the first HPV159 isolate was obtained, HPV159 was further detected in other muco-cutaneous (4/181, 2.2%), mucosal (22/764, 2.9%), and cutaneous (14/554, 2.5%) clinical samples, suggesting its extensive tissue tropism. However, because very low HPV159 viral loads were estimated in the majority of positive samples, it seemed that HPV159 mainly caused clinically insignificant infections of the skin and mucosa. Using newly developed, highly sensitive HPV159-specific nested PCRs, two additional HPV159 LCR viral variants were identified. Nevertheless, all HPV159 mutations were demonstrated outside important functional domains of the LCR, suggesting that the HPV159 viral variants were most probably not pathogenically different. This complete molecular characterization of HPV159 enhances our knowledge of the genome characteristics, tissue tropism, and phylogenetic diversity of <i>Beta</i>-PVs that infect humans.